Arginine Mimetic Structures in Biologically Active Antagonists and Inhibitors

Mašič, Lucija Peterlin

doi:10.2174/092986706779026101

Cited by 57 publications

(29 citation statements)

References 112 publications

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“…8,9 Therefore, to precisely control biological processes and improve the safety profile, selective inhibition of nNOS over the other two isoforms is important for any potential therapeutic agent. The close similarity of active site structures in all three isoforms 10,11 presents a critical barrier to the design of selective nNOS inhibitors.…”

Section: Introductionmentioning

confidence: 99%

Potent and Selective Double-Headed Thiophene-2-carboximidamide Inhibitors of Neuronal Nitric Oxide Synthase for the Treatment of Melanoma

Huang

Yang

et al. 2014

J. Med. Chem.

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Selective inhibitors of neuronal nitric oxide synthase (nNOS) are regarded as valuable and powerful agents with therapeutic potential for the treatment of chronic neurodegenerative pathologies and human melanoma. Here, we describe a novel hybrid strategy that combines the pharmacokinetically promising thiophene-2-carboximidamide fragment and structural features of our previously reported potent and selective aminopyridine inhibitors. Two inhibitors, 13 and 14, show low nanomolar inhibitory potency (Ki = 5 nM for nNOS) and good isoform selectivities (nNOS over eNOS [440- and 540-fold, respectively] and over iNOS [260- and 340-fold, respectively]). The crystal structures of these nNOS–inhibitor complexes reveal a new hot spot that explains the selectivity of 14 and why converting the secondary to tertiary amine leads to enhanced selectivity. More importantly, these compounds are the first highly potent and selective nNOS inhibitory agents that exhibit excellent in vitro efficacy in melanoma cell lines.

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Section: Introductionmentioning

confidence: 99%

Potent and Selective Double-Headed Thiophene-2-carboximidamide Inhibitors of Neuronal Nitric Oxide Synthase for the Treatment of Melanoma

Huang

Yang

et al. 2014

J. Med. Chem.

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“…11,12 However, the therapeutic control of NO synthesis is difficult because of the challenge to achieve highly selective inhibition of the specific isoforms. 13 Each one of the three isozymes is associated with different functions: nNOS is devoted to neuronal signaling, iNOS to the immune response, and eNOS to smooth muscle relaxation and blood pressure regulation. 14 Therefore, selective inhibition of nNOS over the other isozymes is highly desirable for the treatment of neurodegenerative diseases to avoid undesirable effects related to iNOS and eNOS inhibition.…”

Section: Introductionmentioning

confidence: 99%

Selective Monocationic Inhibitors of Neuronal Nitric Oxide Synthase. Binding Mode Insights from Molecular Dynamics Simulations

Huang

et al. 2012

J. Am. Chem. Soc.

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The reduction of pathophysiologic levels of nitric oxide through inhibition of neuronal nitric oxide synthase (nNOS) has the potential to be therapeutically beneficial in various neurodegenerative diseases. We have developed a series of pyrrolidine-based nNOS inhibitors that exhibit excellent potencies and isoform selectivities (J. Am. Chem. Soc. 2010, 132, 5437). However, there are still important challenges, such as how to decrease the multiple positive charges derived from basic amino groups, which contribute to poor bioavailability, without losing potency and/or selectivity. Here we present an interdisciplinary study combining molecular docking, crystallography, molecular dynamics simulations, synthesis, and enzymology to explore potential pharmacophoric features of nNOS inhibitors and to design potent and selective monocationic nNOS inhibitors. The simulation results indicate that different hydrogen bond patterns, electrostatic interactions, hydrophobic interactions, and a water molecule bridge are key factors for stabilizing ligands and controlling ligand orientation. We find that a heteroatom in the aromatic head or linker chain of the ligand provides additional stability and blocks the substrate binding pocket. Finally, the computational insights are experimentally validated with double-headed pyridine analogs. The compounds reported here are among the most potent and selective monocationic pyrrolidine-based nNOS inhibitors reported to date, and 10 shows improved membrane permeability.

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“…[36] 1996 veröffentlichte Zeneca FXa-Inhibitoren wie 24 (Schema 10) mit einer nur noch schwach basischen Gruppe. [37] Lange Zeit wurde hier irrtümlicherweise die Pyridylpiperidinylgruppe für die basische P1-Gruppe gehalten.…”

Section: Faktor-xa-inhibitorenunclassified

“…[37] Lange Zeit wurde hier irrtümlicherweise die Pyridylpiperidinylgruppe für die basische P1-Gruppe gehalten. [36] Aus einer Röntgen-strukturanalyse mit Trypsin wurde jedoch ersichtlich, dass sich die Chlornaphthylgruppe in der S1-Tasche befindet. Es lag nahe, dass eine vergleichbare Orientierung auch für FXa zutrifft.…”

Section: Faktor-xa-inhibitorenunclassified

Orale, direkte Thrombin‐ und Faktor‐Xa‐Hemmer: Kommt die Ablösung für Warfarin, Blutegel und Schweinedärme?

2011

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Bislang müssen sich Patienten zur Vorbeugung von Thrombosen nach Operationen täglich Heparin spritzen oder müssen zur Schlaganfallprophylaxe bei Vorhofflimmern Vitamin‐K‐Antagonisten vom Cumarintyp einnehmen, die eine geringe therapeutische Breite haben und deren Dosierung regelmäßig überwacht werden muss. Um den Therapiestandard bei thromboembolischen Erkrankungen, wie tiefen Venenthrombosen, Lungenembolien und Hirnschlag bei Vorhofflimmern, zu verbessern, wurde in der letzten Dekade intensiv an neuen, oral wirksamen Thrombin‐ und Faktor‐Xa‐Inhibitoren geforscht. Einige dieser Verbindungen sind bereits auf dem Markt oder befinden sich in fortgeschrittener klinischer Entwicklung; sie könnten den Antikoagulantienmarkt revolutionieren.

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Arginine Mimetic Structures in Biologically Active Antagonists and Inhibitors

Cited by 57 publications

References 112 publications

Potent and Selective Double-Headed Thiophene-2-carboximidamide Inhibitors of Neuronal Nitric Oxide Synthase for the Treatment of Melanoma

Potent and Selective Double-Headed Thiophene-2-carboximidamide Inhibitors of Neuronal Nitric Oxide Synthase for the Treatment of Melanoma

Selective Monocationic Inhibitors of Neuronal Nitric Oxide Synthase. Binding Mode Insights from Molecular Dynamics Simulations

Orale, direkte Thrombin‐ und Faktor‐Xa‐Hemmer: Kommt die Ablösung für Warfarin, Blutegel und Schweinedärme?

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